Date published: 2025-9-13

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PRAMEF4 Activators

PRAMEF4, part of the PRAME (Preferentially Expressed Antigen in Melanoma) family of genes, is a fascinating entity in the arena of molecular biology. Typically, PRAME genes are expressed in the testes and function within the scope of immune evasion during spermatogenesis. However, aberrant expression patterns of PRAMEF4 have been documented in diverse cancer cell lines, suggesting its role extends beyond normal physiological processes. PRAMEF4's exact function remains elusive, but it is considered to play a part in gene expression regulation. The gene's expression in tumors compared to normal tissues has led to a burgeoning interest in understanding the conditions that can influence its expression levels.

Research has indicated that various chemical compounds can potentially act as activators to induce the expression of genes like PRAMEF4. For instance, epigenetic modifiers such as 5-Azacytidine and Decitabine, known for their DNA demethylation effects, could upregulate PRAMEF4 by remodeling the chromatin structure around its promoter to facilitate transcription. Histone deacetylase (HDAC) inhibitors, including Trichostatin A and Vorinostat, might similarly promote a more transcriptionally permissive environment, leading to an increase in PRAMEF4 expression. Compounds such as Retinoic acid and Vitamin D3, which engage with their respective nuclear receptors, could also stimulate the expression of PRAMEF4 as part of a broader modulation of gene networks. Additionally, dietary components like Resveratrol and Sulforaphane, known for their roles in gene expression via various signaling pathways, could potentially induce PRAMEF4 expression. It's important to note that while these compounds are active in cellular pathways, the theoretical induction of PRAMEF4 expression by these chemicals requires empirical validation through rigorous scientific experimentation.

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